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Abstract

Objectives

To conduct a systematic review for the evidence supporting or disproving the reality
of parenteral nutrition- antiepileptic drugs interaction, especially with respect
to the plasma protein-binding of the drug.

Methods

The articles related to the topic were identified through Medline and PubMed search
(1968-Feburary 2010) for English language on the interaction between parenteral nutrition
and antiepileptic drugs; the search terms used were anti-epileptic drugs, parenteral
nutrition, and/or interaction, and/or in vitro. The search looked for prospective
randomized and nonrandomized controlled studies; prospective nonrandomized uncontrolled
studies; retrospective studies; case reports; and in vitro studies. Full text of the
articles were then traced from the Universiti Sains Malaysia (USM) library subscribed
databases, including Wiley-Blackwell Library, Cochrane Library, EBSCOHost, OVID, ScienceDirect,
SAGE Premier, Scopus, SpringerLINK, and Wiley InterScience. The articles from journals
not listed by USM library were traced through inter library loan.

Results

There were interactions between parenteral nutrition and drugs, including antiepileptics.
Several guidelines were designed for the management of illnesses such as traumatic
brain injuries or cancer patients, involving the use of parenteral nutrition and antiepileptics.
Moreover, many studies demonstrated the in vitro and in vivo parenteral nutrition
-drugs interactions, especially with antiepileptics.

Conclusions

There was no evidence supporting the existence of parenteral nutrition-antiepileptic
drugs interaction. The issue has not been studied in formal researches, but several
case reports and anecdotes demonstrate this drug-nutrition interaction. However, alteration
in the drug-free fraction result from parenteral nutrition-drug (i.e. antiepileptics)
interactions may necessitate scrupulous reassessment of drug dosages in patients receiving
these therapies. This reassessment may be particularly imperative in certain clinical
situations characterized by hypoalbuminemia (e.g., burn patients).

Introduction

In the past, many efforts have been made to supply nutrients intravenously through
cannulation of peripheral veins. However, administration of different feeding solutions
like milk, salted water and glucose were associated with thrombophlebitis or fluid
overload [1]. In 1968, Dudrick and his colleagues administered a nutrition solution through the
superior vena cava, enabling the administration of a small volume of nutrition solution
with high nutrient concentrations [2]. The practice of intravenous feeding was then utilised to nourish an infant for more
than 6 weeks. Subsequently, many adult and paediatric patients with gastrointestinal
abnormalities were sustained by nutrition support via a central venous catheter [3,4]. A great advancement has been made in methods for IV cannulation and IV nutrient
liquids formulation during the past four decades. Currently, the IV administration
of complex nutrient mixture is equated with parenteral nutrition (PN) and has become
a vital part of the health management for both outpatients and hospitalised patients
who are not able to eat or consume nutrients through the gastrointestinal tract [1].

The parenteral nutrition technique can be applied to all patients regardless of their
gastrointestinal function or metabolic status. However, many challenges and controversial
issues may be involved in the assessment of beneficial effects gained from IV nutrition
in certain patients [5-9]. Malnutrition has been found to have negative effects on the incidence of postoperative
complications, length of hospitalisation, and mortality [10-20]. A patient's nutritional status can be improved and reinstated by both parenteral
and enteral nutrition [21-32]. Although previous studies have demonstrated a positive effect of nutrition support
on length of hospital stay, morbidity, and mortality [8,18,28,33-36]. A meta-analysis study has revealed that total parenteral nutrition does not have
an effect on the death rate of surgical patients, but it may possibly decrease the
complication rate, particularly in malnourished patients [37]. Consequently, clinicians must consider the general guidelines and clinical judgments
as the basis and structure for deciding the suitability of nutrition support.

Several questions can be considered in deciding whether nutrition support is clinically
beneficial for a given patient [38]:

• Does malnutrition exist?

• Will the malnutrition contribute to an increased likelihood of mortality or morbidity,
or decrease in the response to other therapies?

• Is the existing malnutrition a consequence of starvation, altered metabolism, or
a combination of both?

• Will treating the malnutrition with either enteral or parenteral nutrition result
in an improvement in nutritional status?

• Will an improvement in nutritional status affect morbidity, response to therapy,
or mortality?

• Considering the effect of nutrition support on patient outcome, will the cost of
providing nutrition support outweigh the cost of not providing nutrition support?

A number of aspects have to be considered when assessing a patient's suitability for
nutrition support, including the patient's age, the existence of critical illness,
the occurrence of malnutrition and its severity, and the importance of nutrition support
to the whole therapeutic management plan [39]. The cornerstone that governs the decision on which route of nutrition support should
be utilised in a certain patient is the functional capability of the gastrointestinal
tract. Generally, the enteral route is more favoured than the PN as it consistently
meets the nutrition requirements [40]. However, PN should be used when nutrition requirements cannot be met by enteral
nutrition and when the gastrointestinal tract is not functioning or cannot be accessed.
As with any therapy, patients should be monitored and should undergo thorough routine
evaluations to assess the best route of nutrition support as frequently as possible.

Many types of complications may be associated with the use of PN, such as mechanical
and septic complications related to intravenous catheters. These complications may
be observed directly after placing of a central venous catheter and may include intravascular
and extravascular malposition, hydrothorax, hemothorax, brachial nerve plexus injury
and pneumothorax [41-45]. Thrombosis is considered to be one of the late complications that may happen in
the lumen of the intravenous catheter and may also affect the blood vessel around
the catheter [41-47]. Contaminated IV fluid or contamination of the catheter site may lead to septicaemia,
which is considered to be a serious, life-threatening complication [41-46,48-55]. In addition to the mechanical and septic complications, various sorts of metabolic
complications may be associated with PN. The most frequently reported abnormalities
are hypokalaemia, hypomagnesaemia, hypophosphataemia and hyperglycaemia. Routine monitoring
of these serum electrolytes is very important to identify any electrolyte disturbances
and to avoid any possible complications [56].

Improvement of pharmaceutical safety has been studied in terms of stability and compatibility
for total parenteral nutrition (TPN) admixture [57]. Parenteral drugs should be given separately from TPN solutions. However, sometimes
it is impossible to absolutely dedicate the lumen to administration of TPN, particularly
in ICU and cancer patients. In such patients, the number of IV drugs sometimes exceeds
the number of available access sites [58]. Although intravenous drug-drug incompatibility has been widely discussed [59], information relating to drug-PN incompatibility is limited. The problem is compounded
by the huge variability in nutrition components and concentrations; furthermore, there
are different ranges and concentrations of drugs that may be used [58]. Even though PN plays a significant role in a variety of cases, there are some potential
interactions that might occur with drugs administered concurrently with PN. Therefore,
the goal of this article was to perform a systematic review for the evidence supporting
or disproving the existence of PN- antiepileptic drugs interaction, especially with
respect to the plasma protein-binding of the drug.

The authors conducted Medline and PubMed search from 1968 to February 2010 for English-
language articles describing the interaction between PN and antiepileptic drugs; the
search terms used were anti-epileptic drugs, PN, and/or interaction, and/or in vitro.
The search looked for prospective randomized and nonrandomized controlled studies;
prospective nonrandomized uncontrolled studies; retrospective studies; case reports;
and in vitro studies. Full text of the articles were then traced from the Universiti
Sains Malaysia (USM) library subscribed databases, including Wiley-Blackwell Library,
Cochrane Library, EBSCOHost, OVID, ScienceDirect, SAGE Premier, Scopus, SpringerLINK,
and Wiley InterScience. The articles from journals not listed by USM library were
traced through inter library loan.

Study designs

After performing the required search, a huge lacking of the formal research evidence
was found. So that, this review will mostly depend on the use of anecdotes and case
reports to describe some of the pharmacokinetic issues (mainly plasma protein binding)
of the use anti-epileptic drugs and PN in critically ill patients.

Parenteral nutrition and anticonvulsants in traumatic brain injury

Serious head injury is often followed by hypermetabolism, hypercatabolism, and nitrogen
loss [60,61]. Hypermetabolism is characterised by an increase in the levels of catabolic hormones,
especially cortisol, epinephrine, norepinephrine, and glucagon. Hypermetabolism results
from an elevation in the level of catabolic hormones, cytokines, and catecholamines,
leading to increases in the cardiac output, tachycardia, and mild hypertension. Consequently,
oxygen consumption and caloric requirement will be increased. A hypercatabolic state
is the consequence of amino acid mobilisation from skeletal muscles, gluconeogenesis,
increased nitrogen excretion, loss of weight, and muscle wasting. In addition to the
skeletal muscles, visceral and circulating protein will undergo proteolysis if aggressive
nutritional support is not provided [60,62]. Hypermetabolic and hypercatabolic states can precipitate a condition of severe malnutrition
that leads to several complications, such as poor wound healing, loss of body mass,
immunosuppression, infection, and multiple organ failure [60,63]. Therefore, nutritional support is mainly given to ensure the required calories and
proteins and to achieve a positive nitrogen balance [63]. However, a positive nitrogen balance may not be reached for 2 to 3 weeks after injury,
even with aggressive nutritional support [60,64]. Nutritional therapy is recommended by the Guidelines for the Management of Severe
Head Injury, which state that nutrition support should start within 72 hours of injury
and with complete caloric replacement should be achieved within 7 days [65].

Total parenteral nutrition provides early feeding if enteral nutrition is not accessible
or enteral feeding is not feasible due to gastrointestinal malfunction. Total parenteral
nutrition provides a steadier nutritional intake and causes less diarrhoea than enteral
nutrition [63].

Seizure is one of the most common posttraumatic complications in patients with a recent
head or brain injury [66]. Jennett confirmed that the severity of a brain injury can be used to estimate the
probability of early (within 7 days of injury) and late (after 7 days) risk of seizures
[67]. Annegers and colleagues have demonstrated that a small increase in the risk of epilepsy
may be noted in subsequent years with mild (loss of consciousness or amnesia for less
than 30 minutes) and moderate brain injuries (loss of consciousness, amnesia for 30
minutes to 24 hours, or skull fracture). In addition, a significantly increased risk
of epilepsy is associated with more severe brain injuries (loss of consciousness,
amnesia lasting for more than 24 hours, subdural haematoma, or brain contusion) over
the next 10 years [68]. A systematic review of ten randomised controlled trials revealed consistent evidence
regarding the early management with anticonvulsant drugs after head injury. Phenytoin
is the gold standard; however, phenobarbital and carbamazepine also reduced the relative
risk of early seizures [69]. Moreover, valproic acid was suggested as an alternative agent for posttraumatic
seizure prophylaxis; however, patients receiving valproic acid had a slightly higher
mortality rate than those receiving other antiepileptic drugs [70].

Parenteral nutrition and anticonvulsants in cancer patients

Many review articles and meta-analysis studies have been published to evaluate the
effects of nutritional support in cancer patients. In this sequence, a consensus has
been made to create standards for nutritional support in cancer patients [71]. Klein et al. utilised 28 randomised controlled trials to evaluate the use of PN
in cancer patients. They concluded that the use of PN in patients with cancer of the
gastrointestinal tract is justified. Although the risk of infection increased in patients
receiving both PN and chemotherapy, the authors did not rule out the potential benefit
of PN in cancer patients treated with radiotherapy and chemotherapy [72]. Another review article including 12 randomised controlled trials was published by
the American College of Physicians. The aim of this review was to predict the effect
of PN on survival and tumour response rate in patients undergoing chemotherapy. The
findings of the pool analysis revealed that the tumour response rate was not improved
by PN and that there was no significant difference between the control patients and
those who received PN in terms of the survival rate [73]. The American Society for Parenteral and Enteral Nutrition (ASPEN) recommended the
following practice guidelines [74]:

• Enteral and parenteral nutrition may have positive effects in some severely malnourished
cancer patients or those who are unable to take adequate oral nutrition for more than
one week. Patients under this category should be given nutrition support, if possible,
in concurrence with the start of oncologic therapy.

• Nutritional support is not routinely recommended for mildly malnourished or well-nourished
patients and those who are able to receive adequate nutrition via oral intake, even
if they are undergoing chemotherapy, radiotherapy, or surgery.

• Total parenteral nutrition may have an invaluable effect in the management of patients
with advanced cancer that are identified as unresponsive to radiation therapy or chemotherapy.

Furthermore, a prospective evaluation of quality of life in one hundred forty-six
patients with head and neck cancer was reported [75]. The results revealed that nutrition support should be applied in cancer patient
because its positive effects can improve the overall quality of life. In addition
to nutritional support, anticonvulsant drugs may be incorporated in the treatment
of cancer patients because seizure is a common neurological complication in patients
with primary brain tumours and brain metastases [76,77]. A large discrepancy in seizure frequency was noted between patients with different
primary brain tumours and patients with cerebral metastases from various primary tumours
(Table 1) [77].

Table 1. Seizure frequency within different primary brain tumours and within cerebral metastases
from various primary tumours

The majority of brain tumour patients need chronic treatment with antiepileptic drugs
because seizures are common in this population of patients. Sometimes, prophylactic
use and acute treatment with antiepileptic drugs might be necessary [77]. Actually, clinicians follow general guidelines for the acute therapeutic management
of seizures in patients with both epilepsy and brain tumours, including intravenous
benzodiazepines, valproic acid, and levetiracetam, followed by phenytoin and then
barbiturate if necessary [78]. Older generations of antiepileptic drugs (phenytoin, carbamazepine, and oxcarbazepine)
are hepatically metabolised and induce cytochrome P450, which can reduce the efficacy
of chemotherapeutic agents. New generations of antiepileptic drugs might be more convenient
for the chronic treatment of seizures in cancer patients in relation to the induction
of liver enzyme [77].

Valproic acid is a broad-spectrum antiepileptic drug that has been considered as a
safe and potent drug for many decades. Recently, many studies have shown that valproic
acid has some anticancer properties [79-81]. However, further studies are required to evaluate the efficacy and safety of valproic
acid; not only as an antiepileptic drug, but also as a potential anticancer drug in
patients with brain tumours [77]. Although prophylactic administration of anticonvulsant drugs is evidence-based in
some circumstances, it is not recommended and might not be effective at preventing
the first seizure [76,77].

Systematic categorisation of drug-nutrient interactions

Interactions between drugs and nutrients frequently occur and might have a negative
impact on the patient's clinical outcome [82]. These interactions became more relevant with the dramatic development of nutrition
support and with the increased use of multiple medications. Identification of clinically
important interactions can help in avoiding or early management of adverse effects
resulting from drug-nutrient interactions. This point was emphasised by the Joint
Commission on Accreditation of Healthcare Organizations (JCAHO) through its standards
that encourage clinicians to monitor any potential interactions between drugs and
nutrients [83]. Based on the current information required for recognition and suitable management
of drug-nutrient interactions in patients receiving parenteral and enteral nutrition,
drug-nutrient interactions were sorted into four types [84]:

• Ex vivo biopharmaceutical inactivations

• Interactions affecting the absorption phase

• Interactions affecting systemic/physiologic dispositions

• Interactions affecting elimination/clearance

Ex vivo biopharmaceutical inactivations

The contact between drug molecules and nutritional constituents that leads to physical
or biochemical reactions may occur through ex vivo biopharmaceutical interactions. These interactions typically happen outside the body,
either in the delivery system (e.g., infusion bags or infusion tubings) or during
the compounding process. Several examples are available for this type of interaction,
such as the physical incompatibility between PN fluid and intravenous drugs, the hydrolysis
reaction that results from the direct mixing of oral liquid drugs with enteral feeding
formula, and the destruction of fat emulsion that occurs when a large quantity of
heparin is added into 3-in-1 parenteral nutrition formula. Crystals, precipitates
or other undissolvable intermediates may result from these interactions as a final
byproduct. Life-threatening events (e.g., occlusion of blood vessels) may occur from
the systemic exposure of the patient to these byproducts. On the other hand, physical
incompatibility with enteral nutrition usually does not cause life-threatening conditions,
but it may result in a decrease in the therapeutic effect or poor nutritional improvement
[84]. One of the common examples that can be seen is the dramatic reduction in the phenytoin
absorption when given with enteral nutrition [85,86].

Absorption interactions

Absorption interactions can occur with drugs and nutrients that are only taken or
delivered orally or through enteral feeding delivery systems. The oral bioavailability
of the active drug may increase or decrease as a result of these interactions [84]. Absorption interactions can be subclassified into the following three types: 1)
presystemic metabolism (e.g., grape fruit juice with carbamazepine) [87], 2) presystemic transport (e.g., vitamin E and cyclosporine) [88], and 3) presystemic binding/complexation (e.g., tetracycline binding to divalent
cations in the gastrointestinal tract) [89].

Interactions affecting systemic or physiologic dispositions

This type of interaction occurs after the drug molecule or the nutritional constituent
has reached the systemic circulation. It might be observed as an alteration in tissue
distribution, systemic metabolism, or penetration into a specific tissue. In some
clinical situations, the interaction between the drug and the nutrient element may
be mediated by cofactors or hormones [84]. One example of this phenomenon is the reduction in the anticoagulant effect of warfarin
with a vitamin K-rich diet [90]. Intravenous fat emulsions are supplementary resources of vitamin K and have been
correlated with warfarin resistance when used in combination with intravenous nutrition
or as delivery system for propofol [91].

Interactions affecting drug elimination or clearance

This type of interaction influences either hepatic metabolism or renal elimination
of the object agents via the involvement of precipitant agents. Numerous pathways
may be involved, such as the antagonism, modulation, or diminishment of renal or enterohepatic
transportation [84]. High protein diets have been seen to enhance the hepatic elimination of certain
drugs like propranolol [92]. The use of aminoglycosides in malnourished patients may be considered as another
example of these interactions. Both the volume of distribution and the extracellular
fluid compartment may show a significant expansion due to a decrease in the lean tissue
mass. Therefore, dosing adjustment of aminoglycosides in malnourished patients must
be matched with any alteration in the volume of distribution in order to achieve the
appropriate therapeutic drug concentrations [93].

Nutrient-antiepileptic drugs interactions

Similar to haemoglobin, albumin undergoes an in vivo non-enzymatic glycosylation; in fact, approximately 6-10% of the total serum albumin
is glycosylated in healthy adult. A group of investigators found that the binding
affinities for long chain fatty acid and bilirubin were lower when the glycosylation
of albumin was increased [94]. Zimmerman et al. reported that an increase in the concentration of free fatty acids
in serum led to an increase in the free fraction of valproic acid [95]. Doucet et al. observed that phenytoin protein binding was significantly decreased
in sera from diabetics, but there was no correlation between the percentage of binding
and the concentration of glycated albumin [96]. Moreover, Dutkiewicz et al. demonstrated that in hypercholesterolemia and in mixed
hyperlipidemia, the free phenytoin concentration was increased. This effect was most
likely correlated with the displacement of phenytoin by free fatty acids [97,98]. Accordingly, the free fatty acids from fat emulsions in TPN fluid could displace
phenytoin or other drugs from their albumin-binding sites.

Previous studies have shown that drug binding to site II of human serum albumin can
be significantly altered by L-tryptophan in amino acid fluids. Because phenytoin can
react with site II of human serum albumin [99], these findings are substantially useful for evaluating the pharmacokinetic and pharmacodynamic
effects of phenytoin or other therapeutic drugs in patients receiving TPN or a parenteral
nutrition solution with amino acids [100]. Furthermore, a decrease in the total phenytoin concentration was reported in a 40-year-old
man who started TPN therapy concurrently with phenytoin; the total phenytoin concentration
subsequently increased to the pre-TPN concentration following the cessation of TPN
therapy [101]. The competitive binding of selected therapeutic drugs to five PN formulas and to
human serum in vitro has been evaluated using equilibrium dialysis. Phenytoin, phenobarbital, and valproic
acid were found to be bound less in the presence of PN than human serum (Table 2), suggesting that the free fraction of these drugs might increase in vivo in the presence of these fluids [102].

Table 2. Differences in binding of some antiepileptic drugs to parenteral nutrition fluids
and to human serum

Alteration of plasma protein binding of antiepileptic drugs

Several factors have been shown to alter the binding of antiepileptic drugs to plasma
protein, including hypoalbuminaemia (patients with burns, old age, pregnancy, AIDS
etc.) [103,104]; patients with uraemia [105]; drug-drug interactions; displacement of the drug from its plasma protein binding
by another drug [106,107]; and patients with chronic liver disease [108].

In vitro and in vivo studies have been done to observe the displacement of phenytoin from its protein-binding
site by antibiotics. The results showed that ceftriaxone, sulfamethoxazole, and nafcillin
could all displace phenytoin from serum protein carriers [109].

The effect of albumin and α-1-acid glycoprotein on the binding of therapeutic drugs
has been determined by Bailey and Briggs. Their study showed that increasing the concentration
of α-1-acid glycoprotein will increase the degree of phenytoin binding by 3-fold,
whereas decreasing albumin concentration will decrease the binding by less than 1.2-fold.
Phenobarbital and valproic acid exhibited an elevation in their free level when albumin
concentration was reduced. Ultimately, conditions like acute inflammation that increase
α-1-acid glycoprotein may result in a decrease in the free phenytoin concentration
which would not be significantly offset by the decease of albumin levels [110].

Albumin binding sites

Pharmacokinetics are crucially directed by drug-protein binding in the blood that
involve transportation, metabolism and elimination of many pharmaceutical agents.
This type of binding can also be a starting place for drug-drug interactions [111-113]. Consequently, it is important to have good knowledge about the type and number of
binding sites that a certain drug will interact with on a given protein because this
information allows us to estimate how this agent will be influenced by other substances.

Albumin is considered to be the most important plasma protein that is involved in
such interactions. The warfarin-azapropazone site (Sudlow Site I) and the indole-benzodiazepine
site (Sudlow Site II) are the two major albumin binding sites for drugs [114]. Additionally, there are several minor binding sites on albumin for various drugs
such as digitoxin and tamoxifen [115,116]. High performance affinity chromatography was used to study the binding of phenytoin
to albumin. This study found that phenytoin can interact with albumin at the warfarin,
benzodiazepine, tamoxifen and digitoxin sites of this protein (Figure 1) [99]. Dasgupta and Timmerman have studied the in vitro phenytoin displacement from protein binding by some non-steroidal anti-inflammatory
drugs in both normal and uremic sera. The results illustrated that free phenytoin
levels were significantly increased with ibuprofen in both normal and uremic sera
[117]. Due to the re-equilibrium phenomena, the in vivo situation might be slightly different.
The free phenytoin concentration may not change; it is the free fraction that changes.
Ibuprofen-phenytoin interactions can be predicted from their albumin binding sites.
Kragh-Hansen et al. showed that ibuprofen is a selective drug probe for site II of
human serum albumin [118].

Figure 1.Proposed model for phenytoin binding to HSA. The data in this report is consistent with a model in which phenytoin has direct
binding at both the warfarin-azapropazone and tamoxifen sites, although it is possible
that the competition noted in this study could have been due to negative plus positive
allosteric effects between this drug and R-warfarin or cis-clomiphene. From Chen et al. (2004) [99] with permission of the authors and the publisher.

Monitoring free drug concentrations

Many drugs bind to various plasma proteins (albumin & α-1-acid glycoprotein). This
protein binding can be low, moderate or high (>80%). Some drugs, such as ethosuximide
and lithium, don't bind to any plasma proteins [119]. Protein binding of most monitored therapeutic drugs is shown in Table 3[108]. Reversible equilibrium and law of mass action govern the existence of drugs in the
peripheral circulation as free (unbound) and bound to proteins. Only free drug can
produce the pharmacological action by crossing the plasma membrane and binding with
the receptors [119]. In addition, the free drug component can freely cross blood-CSF or blood brain barriers
[120]. In general, drugs that highly bind plasma proteins are the most important candidates
for monitoring of free drug concentrations because variation in protein binding may
produce a clinically noteworthy effect in altering free drug concentrations. Newer
drugs such as mycophenolic acid, mofetil and certain protease inhibitors are considered
to be good candidates for monitoring free drug concentrations. However, free drug
concentrations of the old generation of antiepileptic drugs such as phenytoin, carbamazepine
and valproic acid are still the most requested by clinicians [108].

Old generation antiepileptic drugs

Traditional antiepileptic drugs such as valproic acid, carbamazepine and phenytoin
are highly bound to protein. The clinical usefulness of monitoring free concentrations
of those drugs has already been studied and documented. Furthermore, the external
survey specimens of the College of American Pathologists have also listed the free
anticonvulsant concentrations, and assay kits for measurement of free concentrations
of these drugs are commercially available [108].

The plasma protein binding of valproic acid ranges from 90 to 95% and occurs mainly
with albumin [121]. Because of the saturable binding phenomenon, valproic acid shows vacillation in
its protein binding within the therapeutic range (50-100 μg/ml), leading to fluctuation
of the free fraction from 10 to 50% [122]. Moreover, several studies revealed that there is no correlation between therapeutic
response to valproic acid and its total serum concentration [123,124]. Meanwhile, free valproic acid concentration has been demonstrated to have clinical
benefit in the management of epilepsy and the evasion of unwanted side effects [125]. The significance of monitoring free valproic acid in a heart transplant recipient
with hypoalbuminaemia has been shown in a case report by Haroldson et al. After the
dosing adjustment of valproic acid was based on free concentration rather than total
concentration, the patient improved and was finally discharged from the hospital [126]. A case of neurotoxicity has been reported by Gidal et al., in which a hypoalbuminaemic
patient exhibited a drastic increase in the plasma free valproic acid concentration
with a relatively normal total concentration [127].

In addition, interindividual variation of total valproic acid plasma concentration
and its tendency to underrate the effect of poor compliance was observed, but great
advantages can be derived by depending on free valproic acid concentration instead
of total concentration in therapeutic drug monitoring [128].

Phenytoin is a narrow therapeutic index anticonvulsant drug that appears to follow
the Michaelis-Menten pharmacokinetics [129,130]. Approximately 90% of plasma phenytoin is bound to serum albumin [129]. Therapeutically, phenytoin plasma concentrations range from 10-20 μg/ml, which is
representative of the total phenytoin concentration [131,132]. Free phenytoin was reported by Soldin to be the most requested measurement of free
drug level by clinicians. It was found to be more reliable for the prediction of phenytoin
therapy than the total concentration because only free molecules can pass through
the blood brain barrier and produce the therapeutic effects [133].

In a retrospective study conducted in Japan by Iwamoto et al. [134], they investigated the relationship between the total or free phenytoin concentration
and clinical response, as well as the factors that influence free phenytoin concentration.
The study demonstrated that free phenytoin concentrations were poorly correlated with
total phenytoin concentrations in both monotherapy and multidrug therapy patients.
Free phenytoin concentrations were found to be strongly correlated with the [total
phenytoin]/[serum albumin] ratio in patients receiving monotherapy. However, no significant
correlation was seen between the free phenytoin concentrations and the [total phenytoin]/[serum
albumin] ratio in patients receiving multidrug therapy.

Patients were classified according to their clinical response into the following three
groups: complete response, partial response and no response. There was no significant
difference among the three groups in the total and free phenytoin concentration in
patients receiving multidrug therapy. While the total phenytoin concentration tended
to be higher in the complete response group than in the partial response group in
monotherapy patients, the difference was not statistically significant. On the other
hand, free phenytoin concentrations were significantly higher in the complete response
group than in the partial response group of patients receiving monotherapy.

Both the mean serum albumin and the mean creatinine clearance were significantly lower
in patients with a high free fraction of phenytoin. However, there was no significant
correlation between creatinine clearance and serum albumin levels. Therefore, the
effect of creatinine clearance levels on phenytoin protein binding is unrelated to
the serum albumin levels. At the same time, the mean age was significantly higher
in patients with a high free fraction of phenytoin than in those with a normal or
low free fraction. Moreover, Banh et al. have observed that most phenytoin toxicities
developed in patients with normal or low total phenytoin concentrations, but with
an elevated free concentration of phenytoin [135].

New generation antiepileptic drugs

In the last two decades, several new antiepileptic drugs have been commercially introduced
in the United States and/or Europe. These drugs are tiagabine, eslicarbazepine acetate,
stiripentol, felbamate, rufinamide, gabapentin, pregabalin, lacosamide, oxcarbazepine,
lamotrigine, topiramate, levetiracetam, vigabatrin and zonisamide. It is well documented
that these newer agents exhibit better clinical characteristic (i.e. less sever adverse
effect and broader therapeutic range) than the older antiepileptic drugs. Similar
to the traditional antiepileptics, some of the newer agents may also be indicated
for other clinical situations such as chronic pain syndromes and bipolar disorder
[136-138]. Most of the newer agents show little binding to plasma protein (Table 3) [108,139]. However, some of the new antiepileptic drugs do not have any affinity to plasma
protein like gabapentin, levetiracetam, pregabalin, and vigabatrin. Only two of the
newer antiepileptic drugs (i.e. tiagabine and stiripentol) are considered highly plasma
protein binding [139].

Tiagabine has well documented in several observational studies and case reports to
cause non-convulsive status epilepticus [140-142]. Presently, tiagabine is rarely used in the United States and Europe [136]. Tiagabine is highly plasma protein binding drug (> 96%). Displacement of tiagabine
from its plasma protein binding sites may occur by valproic acid, causing elevation
in the free tiagabine concentration [143]. Clinically, a reference range of 20-200 ng/ml has been designed for tiagabine [144]. Numerous analytical approaches are available for the measurement of tiagabine plasma
concentration such as HPLC and GC/MS [145,146]. However, with some assays not attaining a low enough limit of sensitivity. The measurement
of free tiagabine concentration has been a challenging problem [147].

Stiripentol is one of the new antiepileptic drugs that is highly protein bound (>99%).
It was approved in Europe in 2001 [139]. Even though, stiripentol serum concentration of 4-22 mg/L correlates with control
of absence seizure in childhood. A clear therapeutic range for stiripentol is not
well-proposed [148]. Stiripentol typifies complicated pharmacokinetic characteristics (extensive metabolism,
non-linear pharmacokinetics, and highly plasma protein binding) similar to those of
the old antiepileptic drugs phenytoin [149]. Attention should be given when stiripentol is used with other antiepileptic drugs
like carbamazepine, clobazam, phenobarbital, phenytoin, and valproic acid not only
for the displacement from the plasma protein, but for the inhibitory effect of stiripentol
on the liver metabolizing enzyme of these drugs and/or metabolites as well [150,151].

Several equations were developed to estimate the free phenytoin concentrations from
the measured total phenytoin concentrations and albumin concentrations. Beck et al.
investigated the reliability of different equations for predicting free phenytoin
concentrations. The authors compared the estimated free concentrations with the measured
values. The following three equations were involved in this study: the Gugler method,
the Sheiner-Tozer equation and the Sheiner-Tozer nomogram. The results show that all
three equations for estimating free phenytoin concentrations were unreliable and carried
a lot of bias in predicting free phenytoin concentrations [152]. Furthermore, use of the Sheiner-Tozer equation was not dependable for directing
therapy in critically ill paediatric patients [153]. Accordingly, direct measurement of free phenytoin concentrations is preferred to
the prediction of free phenytoin concentrations using mathematical equations.

Assay techniques for free drug concentrations

The most commonly used method for measuring the free concentration of drugs is equilibrium
dialysis, in which an appropriate buffer and a sample (containing drug and protein)
are separated by a semipermeable membrane. At equilibrium, free drug concentration
is the same in the both chambers (in the sample compartment and in the buffer compartment).
After dialysis, the total drug concentration is lower than in the early sample (due
to dilution). This may lead to serious complexities in the process of result interpretation,
especially when the protein binding depends on the drug concentration (i.e., nonlinear
binding) [154-156]. Equilibrium dialysis is not practical for clinical implication; therefore, ultrafiltration
has become the most preferable technique for monitoring free drug concentrations in
clinical laboratories. A small volume of serum (0.8-1.0 ml) is centrifuged for 15-20
minutes to get the ultrafiltrates. Then the concentrations of free drug are determined
in the protein free ultrafiltrates [108]. The length of centrifugation time is essential for determining free drug concentration.
Liu et al. found that there is a considerable difference between free valproic acid
concentrations in the ultrafiltrate when samples were centrifuged samples for 5 minutes
compared to 10 minutes or 20 minutes. The authors observed that centrifugation for
5 minutes may not be enough time to yield the actual free concentrations. Therefore,
it is recommended to centrifuge the specimens for at least 15 minutes [157]. McMillin et al. reported that the volume of ultrafiltrates were directly proportional
to the centrifugation time and were inversely proportional to albumin serum concentrations.
Although ultrafiltrate volume was substantially increased with increasing centrifugation
time, the free phenytoin concentration did not change proportionately, meaning that
equilibrium was sustained between the ultrafiltrate and serum held in the ultrafiltration
device [158]. Determination of free phenytoin, valproic acid and carbamazepine concentrations
in the ultrafiltrates can be achieved by immunoassays [108]. Free phenytoin concentration in the protein free ultrafiltrate can also be determined
by liquid chromatography combined with tandem mass spectrometry [159].

Critical analysis of lack of evidence

This review came in touch with the importance and significance of careful monitoring
of free antiepileptic drugs concentration in patients receiving PN. However, a clear
shortage of formal research evidence was found. The wrapping up of this article was
based on several anecdotes and case reports. Subsequently, a careful description of
the number and the type of studies were not presented. According to the evidence-based
approach [160], case report was ranked as the lowest source of evidence to influence the pattern
of the decision makers about the therapeutic alternatives. Mostly because these case
reports and anecdotes are collected in an unsystematic technique. So that, the outcome
of these anecdotes cannot reaches to the level of valid generalizable information
[161]. Clinical practice guidelines are developed in systematic approaches to help practitioners
and patients decisions about the suitable health care for certain clinical situations
[162]. In the same time, these guidelines don't behave as replacement for the role of practitioners
and patients in designing the clinical judgment, but it is considered as integrating
tools, not rules. So that, the potency of anecdotes can be realized in complex clinical
decision phenomena, when there is a limited systematic review of the literature [161].

Enkin and Jadad [163] explained the importance and the influence of anecdotes in making clinical decision,
and Jadad [164] previously revealed the strength of the case report within the evidence-based paradigm.
When the point is going in the same trend, anecdotes and formal research evidence
may support each other, and can have an input on practice far better than could be
attained by either alone. Anecdotes can present research findings in more meaningful
approaches. It can personalize, illustrate, and market the formal research findings
[163,165]. When the research evidence reveals a sense of balance between the beneficial and
adverse effects of a treatment, or when it proposes that the treatment alternatives
are approximately equivalent, anecdotal information besides the value and the preference
of the decision maker can play a significant role to reach the final decision.

In some occasions, the evidence from formal research is not obtainable. In such scenario
the decision maker must choose whether or not there is a necessity to explore for
such evidence. Predominantly, this investigation is not ensured, because the cost
or the efforts need for further exploration might not be justified, especially when
the decisions to be made are too measly or unimportant. In this case anecdotes offer
the most excellent and only information on which the decision can be made. Moreover,
this anecdotal information will enhance the motivation of the researchers to perform
the necessary formal research, and will serve as a basis to provide the hypotheses
for more definitive studies. Sometimes, it might be difficult to implement formal
studies, because the clinical problem may be uncommon or the required studies not
are feasible or attractive to financiers [163].

Depending on what have been mentioned above, the authors of this review used several
case reports and anecdotes as powerful tools and vehicles to motivate the researchers
to perform the necessary formal research evidence.

Conclusions

There was no evidence supporting the existence of parenteral nutrition-antiepileptic
drugs interaction due to the lack of prospective, randomized, controlled trials. However,
alteration in the drug-free fraction resulting from coadministration of PN fluids
may be clinically important and may necessitate scrupulous reassessment of drug dosages
in patients receiving these courses of therapies. This reassessment may be particularly
imperative in patients with certain clinical situations in which there are reductions
in the levels of binding proteins (e.g., burn patients). Most patients who receive
PN may also take some therapeutic drugs, leading to potential interactions that may
contribute to adverse events. Surprisingly, there are very few published studies on
the interaction of PN fluids with therapeutic drugs, and most of them do not focus
on protein binding [102,166-169].

Competing interests

None of the authors have accepted or received any honoraria or promise of future benefits
or any other financial support that may inappropriately influence this work or may
lead to some source of bias in designing, writing and finalizing this review article.

Authors' contributions

All authors have made substantial contributions to the conception of the study, drafting
the article, and final approval of the version to be submitted. MS and MB conceived
and designed the study. MS and AA did the electronic search for the relevant articles
and drafted the manuscript. MB revised and edited the manuscript. MS and AA prepared
the manuscript for publication. All authors have read and approved the final submitted
manuscript.

Acknowledgements

The authors would like to acknowledge the Institute of Postgraduate Studies at the
Universiti Sains Malaysia for their support in carrying out this work through providing
the USM Fellowship and the USM-RU-Postgraduate Research Grant Scheme 1001/PFARMASI/842026.